Effector T cells have a lower ligand affinity threshold for activation than naive T cells

doi:10.1093/intimm/dxg087

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International Immunology, Vol. 15, No. 7, pp. 885-892, July 2003
© 2003 Japanese Society for Immunology

Effector T cells have a lower ligand affinity threshold for activation than naive T cells

Kazuhiko Kimachi¹, Katsuji Sugie² and Howard M. Grey²

¹ The Chemo-Sero Therapeutic Research Institute, Kikuchi Laboratory, Kawabe Kyokushi Kikuchi, Kumamoto 869-1298, Japan ² Division of Immunochemistry, La Jolla Institute for Allergy and Immunology, San Diego, CA 92121, USA

Correspondence to: K. Kimachi; E-mail: kimachi{at}kaketsuken.or.jp
Transmitting editor: D. R. Green

It has been previously established that effector and memoryT cells are more sensitive to antigen stimulation than naiveT cells. In this study, we compared the effect of ligand affinityon the activation of naive and effector T cells derived frompigeon cytochrome c (PCC)-specific TCR transgenic mice by stimulatingthese cells with a variety of ligands with widely differingantigenicity. The data obtained indicated the following. (i)The differences in antigen dose requirements for activationof naive and effector cells widened as the affinity of the antigendecreased. Most dramatically, peptides that were TCR antagonistsfor naive T cells were recognized as agonists by effector Tcells. (ii) While both naive and effector T cells were activatedby the bacterial superantigen staphylococcal enterotoxin A,specific for the transgenic TCR V_ß3 chain, effector,but not naive, T cells were stimulated to proliferate by toxicshock syndrome toxin-1, a superantigen not previously describedto be stimulatory for V_ß3 T cells. (iii) EffectorT cells, but not naive cells, proliferated in response to endogenousself-peptides presented by antigen-presenting cells in a syngeneicmixed lymphocyte reaction. Taken together these data indicatethat effector T cells have a lower affinity threshold for activationthan naive T cells. Further studies demonstrated that the heightenedreactivity of effector T cells to low-affinity ligands declinedprogressively with repeated stimulations by antigen such thatafter repeated stimulation effector T cells were no longer stimulatedby low-affinity ligands but recognized them as TCR antagonistssimilar to naive T cells.

Keywords: cellular differentiation, TCR antagonist

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